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Structure of a designed tetrahedral protein assembly variant engineered to have improved soluble expression

机译:经设计可改善可溶性表达的设计四面体蛋白质装配变体的结构

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We recently reported the development of a computational method for the design of coassembling multicomponent protein nanomaterials. While four such materials were validated at high-resolution by X-ray crystallography, low yield of soluble protein prevented X-ray structure determination of a fifth designed material, T33-09. Here we report the design and crystal structure of T33-31, a variant of T33-09 with improved soluble yield resulting from redesign efforts focused on mutating solvent-exposed side chains to charged amino acids. The structure is found to match the computational design model with atomic-level accuracy, providing further validation of the design approach and demonstrating a simple and potentially general means of improving the yield of designed protein nanomaterials.
机译:我们最近报道了一种用于组装多组分蛋白质纳米材料的计算方法的开发。尽管通过X射线晶体学在高分辨率下验证了四种此类材料,但可溶性蛋白质的低收率却阻止了第五种设计材料T33-09的X射线结构测定。在这里,我们报告了T33-31(T33-09的一种变体)的设计和晶体结构,该变体具有改进的可溶性收率,其得益于重新设计的努力,重点在于将溶剂暴露的侧链突变为带电荷的氨基酸。发现该结构与原子级精度的计算设计模型相匹配,为设计方法提供了进一步的验证,并展示了一种简单且可能通用的方法来提高所设计蛋白质纳米材料的产量。

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